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异位 Reelin 诱导具有正常出生日期依赖性的“内-外”排列的神经元聚集在发育中的新皮层中。

Ectopic Reelin induces neuronal aggregation with a normal birthdate-dependent "inside-out" alignment in the developing neocortex.

机构信息

Department of Anatomy, Keio University School of Medicine, Shinjuku-ku, Tokyo 160-8582, Japan.

出版信息

J Neurosci. 2010 Aug 18;30(33):10953-66. doi: 10.1523/JNEUROSCI.0486-10.2010.

Abstract

Neurons in the developing mammalian neocortex form the cortical plate (CP) in an "inside-out" manner; that is, earlier-born neurons form the deeper layers, whereas later-born neurons migrate past the existing layers and form the more superficial layers. Reelin, a glycoprotein secreted by Cajal-Retzius neurons in the marginal zone (MZ), is crucial for this "inside-out" layering, because the layers are inverted in the Reelin-deficient mouse, reeler (Reln(rl)). Even though more than a decade has passed since the discovery of reelin, the biological effect of Reelin on individual migrating neurons remains unclear. In addition, although the MZ is missing in the reeler cortex, it is unknown whether Reelin directly regulates the development of the cell-body-sparse MZ. To address these issues, we expressed Reelin ectopically in the developing mouse cortex, and the results showed that Reelin caused the leading processes of migrating neurons to assemble in the Reelin-rich region, which in turn induced their cell bodies to form cellular aggregates around Reelin. Interestingly, the ectopic Reelin-rich region became cell-body-sparse and dendrite-rich, resembling the MZ, and the late-born neurons migrated past their predecessors toward the central Reelin-rich region within the aggregates, resulting in a birthdate-dependent "inside-out" alignment even ectopically. Reelin receptors and intracellular adaptor protein Dab1 were found to be necessary for formation of the aggregates. The above findings indicate that Reelin signaling is capable of inducing the formation of the dendrite-rich, cell-body-sparse MZ and a birthdate-dependent "inside-out" alignment of neurons independently of other factors/structures near the MZ.

摘要

哺乳动物发育中的新皮层神经元以“由内而外”的方式形成皮质板(CP);也就是说,更早出生的神经元形成更深的层,而较晚出生的神经元则迁移到现有层的上方,形成更浅层的层。 Reelin 是一种由边缘区(MZ)中的 Cajal-Retzius 神经元分泌的糖蛋白,对于这种“由内而外”的分层至关重要,因为在 Reelin 缺失的小鼠(reeler,Reln(rl))中,层是倒置的。尽管自发现 Reelin 以来已经过去了十多年,但 Reelin 对单个迁移神经元的生物学效应仍不清楚。此外,尽管在 reeler 皮层中缺失了 MZ,但尚不清楚 Reelin 是否直接调节细胞体稀疏的 MZ 的发育。为了解决这些问题,我们在发育中的小鼠皮层中异位表达了 Reelin,结果表明 Reelin 导致迁移神经元的前导过程聚集在 Reelin 丰富的区域,进而诱导它们的细胞体在 Reelin 周围形成细胞聚集。有趣的是,异位的 Reelin 丰富区域变得细胞体稀疏和树突丰富,类似于 MZ,并且较晚出生的神经元迁移到它们的前体细胞上方,朝着聚集物内的中央 Reelin 丰富区域迁移,从而导致了在异位情况下依赖出生时间的“由内而外”排列。发现 Reelin 受体和细胞内衔接蛋白 Dab1 对于聚集的形成是必要的。上述发现表明,Reelin 信号能够诱导形成树突丰富、细胞体稀疏的 MZ 以及神经元的依赖出生时间的“由内而外”排列,而无需 MZ 附近的其他因素/结构。

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